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A Branched SELEX Approach Identifies RNA Aptamers That Bind Distinct HIV-1 Capsid Structural Components. | LitMetric

AI Article Synopsis

  • The HIV-1 capsid protein (CA) has different structural forms during replication, which have unique surfaces for interactions, but their specific functions are not well understood due to technical challenges in studying CA.
  • Researchers developed CA-targeting aptamers through a branched SELEX approach, identifying subsets that bind specifically either to the CA lattice or the CA hexamer.
  • The study evaluated these aptamers to understand binding mechanisms and showcased their ability to purify CA from cell lysates, highlighting their potential as valuable tools for investigating CA's diverse structures.

Article Abstract

The HIV-1 capsid protein (CA) assumes distinct structural forms during replication, each presenting unique, solvent-accessible surfaces that facilitate multifaceted functions and host factor interactions. However, functional contributions of individual CA structures remain unclear, as evaluation of CA presents several technical challenges. To address this knowledge gap, we identified CA-targeting aptamers with different structural specificities, which emerged through a branched SELEX approach using an aptamer library previously selected to bind the CA hexamer lattice. Subsets were either highly specific for the CA lattice or bound both the CA lattice and CA hexamer. We then evaluated four representatives to reveal aptamer regions required for binding, highlighting interesting structural features and challenges in aptamer structure determination. Further, we demonstrate binding to biologically relevant CA structural forms and aptamer-mediated affinity purification of CA from cell lysates without virus or host modification, supporting the development of structural form-specific aptamers as exciting new tools for the study of CA.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11320578PMC
http://dx.doi.org/10.1021/acsinfecdis.3c00708DOI Listing

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